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Journal ArticleDOI

Combined Cytotoxicity Effect of Hyperthermia and Anthracycline Antibiotics on Human Tumor Cells

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TLDR
The data indicate that human tumor cell lines have a substantial variety in heat sensitivity and that not every anthracycline antitumor agent is potentiated by temperature, and that ACM's thermoresponse is unique among anthrACYcline antibiotics studied.
Abstract
The effects of temperature on the anthracycline antibiotics-induced cell kill of DND-1A human malignant melanoma (MM) and DND-39A Burkitt's lymphoma (BL) cell lines were studied by means of a clonogenic assay. The two cell lines differed in sensitivity when exposed to heat: The MM cells were unaffected by hyperthermia (42 degrees C), whereas BL cells were sensitive to this temperature. With the MM cells, hyperthermia potentiated the cytotoxic effects of doxorubicin (ADM), daunorubicin, mitoxantrone (DHAD), and quelamycin but did not enhance that of aclacinomycin (ACM). Conversely, the exposure of cells to the anthracycline compounds at 0 degree C resulted in almost complete disappearance of cell kill effects except with ACM; ACM retained substantial cell kill effects even at the given low temperature. For BL cells, ADM- or DHAD-induced cell lethality was also potentiated by hyperthermia; ACM produced only additive cell kill. At 0 degree C, ACM's effects virtually disappeared. These data indicate that human tumor cell lines have a substantial variety in heat sensitivity and that not every anthracycline antitumor agent is potentiated by temperature. ACM's thermoresponse is unique among anthracycline antibiotics studied. Additionally, it was shown that normothermic cell kill by ADM was not affected by hyperthermic preheating; however, preheating of appropriate duration produced important influence on subsequent hyperthermic ADM-induced cell kill.

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Journal ArticleDOI

Extravasation of systemic hemato-oncological therapies

TL;DR: The proper maintenance of intravenous lines, application of local cooling or warming for certain extravasations, and the use of antidotes to prevent the local toxic action of the extravasated drugs are the basis of medical management.
Journal ArticleDOI

Effects of hyperthermia on DNA repair pathways: one treatment to inhibit them all

TL;DR: This review attempts to summarize the known effects of hyperthermia on DNA repair pathways relevant in clinical treatment of cancer and outlines the relationships between the effects of heat onDNA repair and sensitization of cells to various DNA damaging agents.
Book ChapterDOI

Hyperthermia and Drugs

TL;DR: The pattern of modification of the dose response curves of the drugs and the degree of change of their effectiveness by heat depends on a great variety of factors; not all these are known at present.
Journal ArticleDOI

Antidotes to vesicant chemotherapy extravasations.

Robert T. Dorr
- 01 Mar 1990 - 
TL;DR: Although the incidence of chemotherapy extravasation may be lessened with vascular access devices, it nonetheless, continues to comprise a serious and highly litigious area of oncology practice.
Book ChapterDOI

Experimental and Pharmacokinetic Studies in Intraperitoneal Chemotherapy: From Laboratory Bench to Bedside

TL;DR: Extrapolation of experimental results to clinical practice should be done very carefully, because of the differences between the conditions on the laboratory bench and those in the human body.
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